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药物拮抗和单药优势是由死亡动力学的差异引起的。

Drug antagonism and single-agent dominance result from differences in death kinetics.

机构信息

Program in Systems Biology (PSB), University of Massachusetts Medical School, Worcester, MA, USA.

Program in Molecular Medicine (PMM), University of Massachusetts Medical School, Worcester, MA, USA.

出版信息

Nat Chem Biol. 2020 Jul;16(7):791-800. doi: 10.1038/s41589-020-0510-4. Epub 2020 Apr 6.

Abstract

Cancer treatment generally involves drugs used in combinations. Most previous work has focused on identifying and understanding synergistic drug-drug interactions; however, understanding antagonistic interactions remains an important and understudied issue. To enrich for antagonism and reveal common features of these combinations, we screened all pairwise combinations of drugs characterized as activators of regulated cell death. This network is strongly enriched for antagonism, particularly a form of antagonism that we call 'single-agent dominance'. Single-agent dominance refers to antagonisms in which a two-drug combination phenocopies one of the two agents. Dominance results from differences in cell death onset time, with dominant drugs acting earlier than their suppressed counterparts. We explored mechanisms by which parthanatotic agents dominate apoptotic agents, finding that dominance in this scenario is caused by mutually exclusive and conflicting use of Poly(ADP-ribose) polymerase 1 (PARP1). Taken together, our study reveals death kinetics as a predictive feature of antagonism, due to inhibitory crosstalk between cell death pathways.

摘要

癌症治疗通常涉及联合使用药物。以前的大多数工作都集中在识别和理解协同药物-药物相互作用上;然而,理解拮抗相互作用仍然是一个重要且研究不足的问题。为了富集拮抗作用并揭示这些组合的共同特征,我们筛选了所有被表征为调控细胞死亡激活剂的药物的两两组合。该网络强烈富集拮抗作用,特别是我们称之为“单药优势”的拮抗作用形式。单药优势是指两种药物的组合表现出两种药物之一的拮抗作用。优势来自于细胞死亡起始时间的差异,优势药物的作用时间早于其被抑制的对应药物。我们探讨了伴坏死性药物主导凋亡性药物的机制,发现这种情况下的优势是由聚(ADP-核糖)聚合酶 1(PARP1)的相互排斥和冲突使用引起的。总的来说,我们的研究揭示了死亡动力学作为拮抗作用的预测特征,这是由于细胞死亡途径之间的抑制性串扰。

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